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Can the 'neuron theory' be complemented by a universal mechanism for generic neuronal differentiation

机译:可以通过通用神经元分化的通用机制来补充“神经元理论”吗?

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With the establishment of the 'neuron theory' at the turn of the twentieth century, this remarkably powerful term was introduced to name a breathtaking diversity of cells unified by a characteristic structural compartmentalization and unique information processing and propagating features. At the beginning of the twenty-first century, developmental, stem cell and reprogramming studies converged to suggest a common mechanism involved in the generation of possibly all vertebrate, and at least a significant number of invertebrate, neurons. Sox and, in particular, SoxB and SoxC proteins as well as basic helix-loop-helix proteins play major roles, even though their precise contributions to progenitor programming, proliferation and differentiation are not fully resolved. In addition to neuronal development, these transcription factors also regulate sensory receptor and endocrine cell development, thus specifying a range of cells with regulatory and communicative functions. To what extent microRNAs contribute to the diversification of these cell types is an upcoming question. Understanding the transcriptional and post-transcriptional regulation of genes coding for cell type-specific cytoskeletal and motor proteins as well as synaptic and ion channel proteins, which mark differences but also similarities between the three communicator cell types, will provide a key to the comprehension of their diversification and the signature of 'generic neuronal' differentiation. Apart from the general scientific significance of a putative universal core instruction for neuronal development, the impact of this line of research for cell replacement therapy and brain tumor treatment will be of considerable interest.
机译:随着二十世纪初“神经元理论”的建立,引入了这一非常有力的术语,以命名具有惊人的细胞多样性的细胞,这些细胞通过特征性的结构划分以及独特的信息处理和传播特征而得以统一。在二十一世纪初,发育,干细胞和重编程研究融合在一起,提出了可能与所有脊椎动物以及至少大量无脊椎动物神经元产生有关的共同机制。 Sox,尤其是SoxB和SoxC蛋白,以及基本的螺旋-环-螺旋蛋白起着主要作用,尽管它们对祖细胞编程,增殖和分化的精确作用尚未完全解决。除了神经元发育外,这些转录因子还调节感觉受体和内分泌细胞的发育,从而确定了一系列具有调节和交流功能的细胞。 microRNA在多大程度上有助于这些细胞类型的多样化是一个即将到来的问题。理解编码细胞类型特异性细胞骨架和运动蛋白以及突触和离子通道蛋白的基因的转录和转录后调控,这些基因既标志着三种通讯细胞类型之间的差异,又标志着它们之间的相似性,将为理解这些基因提供关键。它们的多样化和“通用神经元”分化的标志。除了公认的通用核心指令对神经元发育的一般科学意义外,该研究系列对细胞替代治疗和脑肿瘤治疗的影响将引起相当大的兴趣。

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